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一个可存活的拟南芥pex13错义等位基因导致严重的过氧化物酶体缺陷,并减少PEX5与过氧化物酶体的结合。

A viable Arabidopsis pex13 missense allele confers severe peroxisomal defects and decreases PEX5 association with peroxisomes.

作者信息

Woodward Andrew W, Fleming Wendell A, Burkhart Sarah E, Ratzel Sarah E, Bjornson Marta, Bartel Bonnie

机构信息

Department of Biochemistry and Cell Biology, Rice University, Houston, TX, 77005, USA.

出版信息

Plant Mol Biol. 2014 Sep;86(1-2):201-14. doi: 10.1007/s11103-014-0223-8. Epub 2014 Jul 10.

Abstract

Peroxisomes are organelles that catabolize fatty acids and compartmentalize other oxidative metabolic processes in eukaryotes. Using a forward-genetic screen designed to recover severe peroxisome-defective mutants, we isolated a viable allele of the peroxisome biogenesis gene PEX13 with striking peroxisomal defects. The pex13-4 mutant requires an exogenous source of fixed carbon for pre-photosynthetic development and is resistant to the protoauxin indole-3-butyric acid. Delivery of peroxisome-targeted matrix proteins depends on the PEX5 receptor docking with PEX13 at the peroxisomal membrane, and we found severely reduced import of matrix proteins and less organelle-associated PEX5 in pex13-4 seedlings. Moreover, pex13-4 physiological and molecular defects were partially ameliorated when PEX5 was overexpressed, suggesting that PEX5 docking is partially compromised in this mutant and can be improved by increasing PEX5 levels. Because previously described Arabidopsis pex13 alleles either are lethal or confer only subtle defects, the pex13-4 mutant provides valuable insight into plant peroxisome receptor docking and matrix protein import.

摘要

过氧化物酶体是真核生物中分解代谢脂肪酸并将其他氧化代谢过程进行区室化的细胞器。通过设计用于筛选严重过氧化物酶体缺陷突变体的正向遗传学筛选,我们分离出了过氧化物酶体生物发生基因PEX13的一个有活力的等位基因,该等位基因具有明显的过氧化物酶体缺陷。pex13 - 4突变体在光合前发育阶段需要外源固定碳源,并且对原生长素吲哚 - 3 - 丁酸具有抗性。过氧化物酶体靶向的基质蛋白的转运依赖于PEX5受体在过氧化物酶体膜上与PEX13对接,我们发现pex13 - 4幼苗中基质蛋白的导入严重减少,且与细胞器相关的PEX5也减少。此外,当PEX5过表达时,pex13 - 4的生理和分子缺陷部分得到改善,这表明在该突变体中PEX5对接部分受损,并且可以通过增加PEX5水平来改善。由于先前描述的拟南芥pex13等位基因要么是致死的,要么仅导致细微的缺陷,因此pex13 - 4突变体为植物过氧化物酶体受体对接和基质蛋白导入提供了有价值的见解。

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